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pISSN 2383-7837eISSN 2383-7845

Mucosal Schwann Cell Hamartoma in Colorectal Mucosa: A Rare Benign Lesion That Resembles Gastrointestinal Neuroma

Jiheun Han · Yosep Chong · Tae-Jung Kim · Eun Jung Lee · Chang Suk Kang

Department of Hospital Pathology, College of Medicine, The Catholic University of Korea, Seoul, Korea

Journal of Pathology and Translational Medicine 2017; 51: 187-189https://doi.org/10.4132/jptm.2016.07.02

▒ BRIEF CASE REPORT ▒

The term mucosal Schwann cell hamartoma (MSCH) was first proposed by Gibson and Hornick in 20091 to describe a group of neuronal polyps purely composed of S-100–positive Schwann cells, in an attempt to distinguish from true “neuromas” and “neurofibromas.” To our knowledge, only 10 cases have been reported in the literature since it was first described (Table 1). MSCH is currently thought to have no association with any inherited disorder. Herein, we describe a case of MSCH and discuss the morphologic and immunohistochemical features with a differential diagnosis in the gastrointestinal (GI) tract.

CASE REPORT

A 2-mm-sized rectal polyp was found in a follow-up colonos-copy of a 49-year-old male who has no significant family history of other neuronal lesions or inherited syndromes but had a tu-bular adenoma resected 2 years prior (Fig. 1A). On microscopic examination, the rectal polyp showed a poorly circumscribed proliferation of spindle cells in the lamina propria, separating the crypt architecture (Fig. 1B). The cells were uniformly elon-gated, with tapered nuclei and abundant eosinophilic cytoplasm with indistinct cell borders. Nuclear atypia, pleomorphism, or mitosis was not observed (Fig. 1C). On immunohistochemical staining, the cells displayed a strong and diffuse positivity for S-100 in both the nucleus and cytoplasm (Ventana, Roche, Tucson, AZ, USA) (Fig. 1D). In comparison, the cells did not have im-

munoreactivity for c-Kit, CD34, glial fibrillary acidic protein, epithelial membrane antigen (EMA), smooth muscle actin, or neurofilament protein (NFP). Because the spindle cells did not form a discrete mass but rather an interspersed proliferation between normal structures, the lesion was diagnosed as MSCH.

DISCUSSION

A diagnosis of MSCH should be made after exclusion of other lesions that resemble spindle cell proliferation and other neuro-nal tumors. Gastrointestinal stromal tumors, which are the most common spindle cell tumor in the GI tract, can be easily excluded by the characteristic immunoreactivity of c-Kit.

Colorectal neurofibromas are another important differential diagnosis of MSCH because they are also composed of Schwann cells, fibroblasts, perineural cells, and NFP-positive axons and usually form a vague tumor without discrete demarcation. How-ever, they are often associated with neurofibromatosis type 1 (NF1), which is usually accompanied by multiple cutaneous neu-rofibromas. Colorectal lesion as a primary clinical presentation without skin manifestation is also exceedingly rare.1

Mucosal neuromas appear as an ill-defined mass and are com-posed of hyperplastic nerve fibers arranged in an irregularly rami-fying manner.1 In contrast to our case, mucosal neuromas have perineurial capsules, which are often EMA-positive. They are almost always multiple and a part of the multiple endocrine neoplasia syndrome type IIb (MEN2B), of which the most im-portant component is a medullary thyroid carcinoma.

GI ganglioneuromas are most common in colorectal neuronal lesions and reveal hypercellular stroma composed of mainly S-100–positive Schwann cells. They differ from MSCH in that they are mixed with variable numbers of neuron-specific enolase–

Corresponding AuthorChang Suk Kang, MD, PhDDepartment of Hospital Pathology, Yeouido St. Mary’s Hospital, College of Medicine, The Catholic University of Korea, 10 63-ro, Yeongdeungpo-gu, Seoul 07345, KoreaTel: +82-2-3779-1312, Fax: +82-2-2258-1628, E-mail: cskang@catholic.ac.kr

Received: March 14, 2016 Revised: June 2, 2016Accepted: July 1, 2016

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188 • Han J, et al.

positive ganglion cells.1,2 Solitary polypoid ganglioneuromas are not associated with systemic manifestations;3 however, ganglio-neuromatous polyposis and diffuse ganglioneuromatosis are

associated with Cowden syndrome, Juvenile polyposis syn-drome, MEN2B (particularly with diffuse ganglioneuromatosis), and NF1.4

Table 1. Features of Schwann cell hamartoma repoerted in colorectum

Reference YearNo. ofcases

Location Age (yr) Sex Symptom Endoscopic finding

Gibson and Hornick1 2009 26 Predominantly in rectosigmoid colon

Mean 62(46–88)

M:F=10:16

Asymptomatic (most common), diarrhea, lower GI bleeding

Sessile polyp, 1–6 mm (mean, 2.5 mm)

Pasquini et al.6 2009 1 Rectosigmoid colon 60 F Occult blood in the stool Sessile polyp, 5 mmRocco et al.5 2011 1 Sigmoid colon 67 F Asymptomatic Sessile polyp, 3 mmSagami et al.7 2012 1 Sigmoid colon 40 M Occult blood in the stool Many small whitish nodules

in mucosaBae et al.3 2013 1 Descending colon 41 F Asymptomatic Polyp, 8 mmNeis et al.4 2013 1 Sigmoid colon 59 M Underlying ulcerative colitis Polyp, 3 mmFerro de Beca et al.8

2014 1 Sigmoid colon 72 M Asymptomatic Polyp, 5 mm

Klair et al.2 2014 1 Rectum 78 F Abdominal pain and intermittent tenesmus

Polyp, 7 mm along with rectal erythema and inflammation

Kanar et al.9 2015 1 Sigmoid colon 67 M Asymptomatic Polyp, 6 mmBae et al.10 2015 1 Rectum 20 M Abdominal discomfort and

loose stoolsPolyp, 4 mm and scattered tiny polyp-like mucosal elevation

Present case 2015 1 Rectum 49 M Asymptomatic Tiny polyp-like mucosal elevation, 2 mm

M, male; F, female; GI, gastrointestinal.

A

C

B

D

Fig. 1. Schwann cell hamartoma of rectal mucosa. (A) Colonoscopy shows a 2-mm sized tiny polyp-like mucosal elevation without erosion or ulceration. (B, C) Hematoxylin and eosin shows scattered proliferation of bland spindle cells in the lamina propria. (D) Immunohistochemi-cal staining for S-100 displays a positivity of both nucleus and cytoplasm.

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Mucosal Schwann Cell Hamartoma • 189

GI schwannomas are composed of bland spindle cells arranged in vague fascicles. Unlike their counterparts from the central nervous system and peripheral soft tissue, the nuclear palisading, so-called Verocay bodies, are absent, which can be similar to MSCH. However, they have characteristic peripheral lymphoid cuffs and form more demarcated tumors than do MSCH.4,5

Mucosal perineuromas are usually solitary lesions and are char-acterized by a whorled growth pattern of bland spindle cells that expand the lamina propria,5 which are morphologically very similar to MSCH. Unlike MSCH, they have colonic epithelium with serrated architecture and express perineural markers such as EMA, whereas they are negative for S-100 protein.2

Finally, inflammatory fibroid polyps (Vanek’s tumor) can be confused with MSCH. They are composed of stellate or spindle-shaped, bland stromal cells that are arranged in an onion skin-like pattern around blood vessels and mucosal glands.5 They have inflammatory infiltrates dominated by eosinophils, which are not observed in MSCH. Additionally, they are not immunoreac-tive for S-100 and are extremely rare in the colon.

MSCH is a rare benign lesion, and cases with clinical features are summarized in Table 1. Cases are primarily detected as small polyps that range from 1 to 8 mm (mean, 5 mm) and are pre-dominantly located in the rectosigmoid colon. Patients are typi-cally asymptomatic, and none of the patient cases were associated with an inherited syndrome. The clinical features of this case are similar to those summarized in Table 1.

In summary, MSCH is a rare lesion that can be found inciden-tally during routine colonoscopy. Although there is currently no indication that MSCH is related to inherited syndromes or malignancies, it is important for pathologists to include it in the differential diagnosis of S-100–positive spindle cell proliferative lesions for accurate diagnosis and to prevent aggressive or unnec-essary treatments.

Conflicts of InterestNo potential conflict of interest relevant to this article was

reported.

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